high-grade primary renal leiomyosarcoma - scielo · of high-grade primary renal leiomyosarcoma....
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ORIGINAL ARTICLE
304
High-grade Primary Renal Leiomyosarcoma_______________________________________________Hakan Ozturk 1
1 Department of Urology, School of Medicine, Sifa University, Izmir-Turkey
ABSTRACT ARTICLE INFO______________________________________________________________ ______________________
Objectıve: To investigate the clinical characteristics, prognosis, survival and diagnosis of high-grade primary renal leiomyosarcoma.Materıals and Methods: From January 2003 to April 2013, 10 cases of high-grade primary renal leiomyosarcoma were retrospectively reviewed. We analyzed clinical manifestations, treatment and prognosis of our group and correlated to the literature.Results: Ten cases (five male and five female patients; age range 43–77 years, mean=57±std d:12.3 ) were enrolled. The mean diameter of the tumor masses was 9.35±4.5 cm (range 3-18 cm). 40% of the patients were asymptomatic while the major symptom of 60% patients was lumbar pain. Nephrectomy was performed in 90% of pa-tients. Partial nephrectomy surgery was preferred for only one patient. Pleomorphism and necrosis with high-grade, pink spindle cell cytoplasm were viewed in all patients. All patients were high-grade, pink spindle cell cytoplasm and pleomorfism and necro-sis were observed in all. In an immunohistochemical examination, vimentin was seen in 100%, desmin in 90% and smooth muscle actin in 80% of the patients. CD117 was negative in all patients. All of the cases were followed-up, and the time of survival varied from 6 to 68 months (mean 23.9±std d:20.1). No patient received adjuvant CTx and/or RTx.Conclusıon: High-grade primary renal leiomyosarcomas (LMSs) are rare and highly malignant and the prognosis is poor. Early diagnosis and radical nephrectomy can prolong the patient’s life. Surgery is the main treatment modality for renal (leiomyo-sarcoma) LMS.
Key words:Sarcoma; Kidney; Leiomyosarcoma; Nephrectomy; Diagnosis; Immunohistochemistry
Int Braz J Urol. 2015; 41: 304-11
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Submitted for publication:March 24, 2014_____________________
Accepted after revision:June 23, 2014
INTRODUCTION
Sarcomas account for 0.8 to 2.7% of ma-lignant kidney tumors. Similar to leiomyomas, leiomyosarcomas (LMSs) originate from the smoo-th muscles of the renal capsule, pelvis renalis, calyxes, and blood vessels. In general, LMSs are more common in females and occur in the four-th and sixth decades. LMSs are solitary lesions. The major symptoms include pain, palpable mass, and hematuria. The tumor occurs more frequently on the right side (1). LMSs are generally highly aggressive malignant tumors originating from
the smooth muscles of the soft tissues, and they exhibit a high potential for metastasis. LMSs of the kidney can originate from the renal pelvis, calyxes, renal capsule, and blood vessels of the kidneys. However, the tumors most commonly ari-se from the smooth muscles of the kidney veins (1). LMSs account for 50-60% of kidney sarcomas. The differentiation from the other renal masses is extremely challenging before surgery (2). Among the other urogenital sarcomas, LMSs of the kid-ney are less frequently encountered compared to sarcomas of the prostate and bladder; however, these tumors are associated with poor prognosis
Vol. 41 (2): 304-311, March - April, 2015
doi: 10.1590/S1677-5538.IBJU.2015.02.17
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in terms of survival. LMSs of the kidney can reach large sizes, due to the lack of natural barriers for leiomyosarcomas arising from the mesenchymal components. Sarcomas typically possess a pseu-docapsule. LMS of the kidney is a rare entity with poor prognosis. LMSs account for only 0.12% of all renal malignancies (3).
MATERIALS AND METHODS
PatientsA total of 10 patients, who underwent sur-
gery due to renal mass between January 2003 and April 2013 and who were diagnosed with high grade primary LMS of the kidney, were included in the present study. During this period, radical ne-phrectomy was applied to 389 patients. 15(3.8%) of these patients were diagnosed with leimyosar-coma. 10 (2.5%) cases were high-graded. Ameri-can Joint Committee of Cancer (AJCC) program was used to follow-up the cases. The symptoms at presentation, radiological findings, and immu-nohistochemical features obtained through patho-logical examination were evaluated. The therapies (radiotherapy and/or chemotherapy) and survival of the patients were recorded.
Diagnosis and staging of Primary renal leiomyosarcoma
The pathological diagnosis and grade of the tumor were evaluated according to the classification of the National Cancer Institute (NCI) and French Federation of Cancer Centers Sarcoma Group (FN-CLCC). The histological grade was scored based in the level of differentiation, presence of mitosis, and necrosis in each high power field (4). All patients were found to a have high grade tumor according to this scoring system (Table-1). The immunohisto-chemical examination included staining for desmin, smooth muscle actin (SMA), vimentin, Bcl-2, CD-34, Ki-67, S-100, and CD117. Markers, which were used for immunohistochemical analysis, were used to distinguish especially from renal cell carcino-ma indicating sarcomatoid differentiation, carci-sarcoma and other subtypes of sarcoma. Vimentin is not specific for tumor type. Therefore it is not used in the differential diagnosis. However, it is in favor of tumor cells staining with negative desmin
Table 1 - The distribution of the patients according to the French Federation of Cancer Centers Sarcoma Group (FNCLCC).
Tumor differentiation
Score 1 n=1 10%
Score 2 n=6 60%
Score 3 n=3 30%
Mitotic count
Score 1 (0-9 mitoses per 10 HPF+) n=0 0%
Score 2 (10-19 mitoses per 10 HPF) n=4 40%
Score 3 (≥ 20 mitoses per 10 HPF) n=6 60%
Tumor necrosis
Score 0 ( no necrosis) n=2 20%
Score 1 (<50% tumor necrosis) n=6 60%
Score 2 (≥50% tumor necrosis) n=2 20%
Histologic grade
Grade 1(total score 2,3) n=3 30%
Grade 2 ( total score 4,5) n=3 30%
Grade 3 ( total score 6,7,8) n=4 40%
with cytokeratin and positive with smooth muscle actin(SMA). Cytokeratin positivity with absence of myoid markers supports a diagnosis of sarco-matoid renal cell carcinoma. Sarcomatoid carci-nomas, however, are not uniformly positive for cytokeratins and may express SMA. Some leio-myosarcomas may also express cytokeratin and or epithelial membrane antigen (EMA). In the latter situation, the presence of desmin is diagnostically helpful since it is positive in leiomyosarcoma and not in sarcomatoid carcinoma (5). The staging of the tumor was based on the system developed by the American Joint Cancer Committee (AJCC-2013) on the staging of soft tissue sarcomas.
Statistical analysisSPSS version 16.0 for Windows was used
for statistical analysis.
RESULTS
The patients included in the study with the diagnosis of high grade primary LMS of the
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Table 2 - Age, gender, clinical appearance, stage, and survival of the cases.
Age Male / Female
Right / Left
Tumordiameter (cm)
Clinical features Stage(AJCC-2013)
Treatment Survival
56 male L 7 (and 3,3,1) lumbar pain T2bN0M0G2
Stage IIB
Radical nephrectomy
9 months
77 male R 8 lumbar pain T2bN0M0G3
Stage III
Radical nephrectomy
15 months
43 female L 3.5 asymptomatic T1bN0M0G1
Stage IA
Partial nephrectomy
44 months
65 female L 3 asymptomatic T1bN0M0G2
Stage IIA
Radical nephrectomy
68 months
49 male R 13(and 5) lumbar pain,hematuria
T2bN1M0G3
Stage III
Radical nephrectomy
7 months
45 male R 18 Lumbar pain, nausea, weight
loss
T2bN1M0G3
Stage III
Radical nephrectomy
6 months
46 female L 10 asymptomatic T2bN0M0G2
Stage Iıb
Radical nephrectomy
23 months
66 female L 13 lumbar pain T2bN1M0G2
Stage III
Radical nephrectomy
8 months
73 male R 6 asymptomatic T2bN0M0G1
Stage Ib
Radical nephrectomy
23 mnoths
50 female L 8 lumabr pain, dyspepsia
T2bN0M0G2
Stage IIb
Radical nephrectomy
36 months
kidney were followed for 6-68 months (mean; 23.9±std d:20.1, Median; 19.0).
Clinical featuresThe mean age was 57 years (range: 43-77
years mean=57±std d:12.3) and the male/female ratio was 1/1. The most common symptom was lumbar pain occurring in 60% (n=6) of patients. Of the patients, 40% (n=4) were asymptomatic, and only 10% (n=1) had hematuria, and 20% (n=2) had systemic and gastrointestinal symptoms (Table-2). According to the staging system of the
AJCC-2013, 40% (n=4) of the patients had a stage III tumor, 30% (n=3) had a stage IIb tumor, 10% (n=1) had a stage IIa tumor, 10% (n=1) had a stage Ib tumor, and 10% (n=1) had a stage Ia tumor. The mean diameter of the tumor masses was 9.35±4.5 cm (range 3-18 cm) (Figures 1-3).
Immunohistopathological FindingsThe immunohistochemical examination
revealed positive staining for desmin (90%, n=9), SMA (80%, n=8), and vimentin (100%, n=10) (Figu-res 4-6). All patients exhibited negative staining for
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Figure 1 - Magnetic Ressonance Imaging: Leiomyosarcoma in pelvis renalis of left kidney (arrow).
Figure 2 - Magnetic Ressonance Imaging: Leioyosarcoma in pelvis renalis of left kidney (arrow).
Figure 3 - Surgical specimen; Left renal leiomyosarcoma (arrow).
Figure 4 - Hematoxilyn-eosin staining demostrat-ing high-grade sarcomatoid cells. H&E [100, 200x] Pleomorfism(small figure) and necrosis (arrow).
Figure 5 - Immunohistochemistry showing Desmin[200x].
Figure 6 - Immunohistochemistry showing difuse actin expression in smooth muscle fiber cytoplasm. Actin[200x].
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Bcl-2. The Ki-67 proliferation index was positive in 60% (n=6) of the patients. All patients showed negative staining for Bcl-2 and CD117 (Table-3).
Treatments and SurvivalNinety percent of the patients (n=9) un-
derwent radical nephrectomy, and 10% (n=1) un-derwent partial nephrectomy. The mean disease--related survival was 23.9±20.1 months (range: 6-68 months), and none of the patients received adjuvant chemotherapy and/or radiotherapy.
DISCUSSION
The incidence of the primary leiomyosar-coma of the kidney increases with age, and this tumor is more common in females than in males and more common in the right kidney than in the left kidney (6). The tumor becomes symptomatic only with the expansion of the tumor size. The symptoms increase with the advancing disease stage. The compression on the neighboring tissues results in lumbar pain and hematuria and the fin-ding of palpable mass on examination; systemic symptoms can also occur, such as nausea, vomi-ting, and abdominal pain (6).
It is extremely challenging to differentiate LMS of the kidney from renal cell cancer exhi-biting sarcomatoid differentiation. These two tu-mors exhibit similar clinical, radiological, and pa-thological features. The most prominent features
that differentiate sarcomas from renal cell cancer are that sarcomas originate from the capsule or perisinous region and sarcomas expand to large sizes without lymphadenopathy, and the lesion contains components such as liposarcoma and os-teosarcoma. These tumors are avascular lesions, with the exception of hemangiosarcomas. The sar-comas should definitely be considered in the diffe-rential diagnosis in the presence of fast-growing renal masses. The sarcomas possess a pseudocap-sule; however, these capsules do not represent a reliable barrier from the surgical point perspecti-ve. The capsule is often found to be infiltrated by the tumor. In general, high grade LMSs show high metastatic potential. Complete surgical resection is the most effective means of therapy (1). The-refore, early diagnosis and early surgical therapy prolong survival in patients with primary LMS. In the present study, the diagnosis and treatment of high grade LMSs and mean survival were discus-sed together with the literature data.
Life expectancy is lower with the sarco-mas of the kidney compared to the other sarcomas of the urinary tract. The 5-year survival is 82% in patients with retroperitoneal sarcoma, 73% in patients with the sarcomas of the bladder, 44% in patients with prostate sarcoma, and 39% in pa-tients with the sarcomas of the kidney (7). Accor-ding to Geonseok et al. the 5-year survival was 51.4% in all of the urogenital sarcomas (7). There are two studies in the literature supporting these
Table 3 - The immunohistochemical features of the cases.
Immunohistochemicalantibody Positive Negative
Desmin (n=9), 90% (n=1), 10%
Smooth muscle actin (SMA) (n=8), 80% (n=2), 20%
Vimentin (n=10), 100% 0%
Bcl-2 0% (n=10), 100%
CD-34 (n=1), 10% (n=9), 90%
*Ki-67 (n=6), 60% (n=4), 40%
S-100 (n=2), 20% (n=8), 80%
CD117 0% (n=10), 100%
*Ki-67 proliferation index ranged between 3% and 70% in the positive cases.
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findings. These studies reported a mean survival around 50% (8, 9). The surgical resection was the most significant prognostic factor in these pa-tients. Lewis et al. reported that the presence of unresectable disease and incomplete surgical re-section were the most significant factors predic-tive of disease-specific death (10). In a study by van Dalen et al., of 143 patients treated in the Netherlands, complete tumor resection was cor-related with better overall survival in the multi-variate analysis (11). The common notion in the literature is that surgical excision was nearly the only prognostic factor in LMSs. There was no cor-relation with the subtypes of the sarcomas and the survival, although statistical evaluation provided limited data due to small number of patients (7). Complete surgical resection with wide margins is the recommended means of therapy in patients with renal LMS. However, the literature also re-ported cases with renal LMS treated with partial nephrectomy (12). In our series, one patient was treated with partial nephrectomy and this patient survived for 44 months, which is higher than the mean survival time. The tumor size being lower than 5 cm is a good prognostic feature (3). In our series, 20% (n=2) of the patients had a tumor me-asuring less than 5 cm. These cases achieved the highest survival rate (44 and 68 months). These findings suggest that small tumor diameter was associated with a good prognosis. In LMS, metas-tasis to the lungs, liver, and colon point to poor prognosis (1). The 5-year survival in patients with sarcoma is around 50% according to the statistical records of the National Cancer Institute (NCI) and AJCC. Vallery et al. reported a survival between 17.9 and 25 months in patients with leiomyosar-coma of the kidney (3). The survival rate of 23.9% in our series was also consistent with the literature data. Although the 5-year mean survival is around 50% in LMS, this rate drops by half in patients with high grade primary LMS of the kidney. This finding suggests that the presence of a high grade tumor decreases life expectancy by half, even if the number of patients was limited in the current cross-sectional study.
In general, it is known that adjuvant/neo-adjuvant chemotherapy/radiotherapy in LMS does not provide survival advantage (1). However, Raut
et al. reported that adjuvant chemotherapy could be used on partially resected tumors (13). Nagumo et al. administered systemic chemotherapy with gemcitabine and docetaxel in a 64-year-old pa-tient with renal LMS and lung metastasis and ob-tained an incomplete response in the lung metas-tasis. The patient developed new metastases in the lungs and pancreas at the end of 29 months. This study is one of the rare reports in the literature the demonstrated the survival benefit of chemothe-rapy, particularly therapy with gemcitabine and docetaxel (14). There are sporadic reports of ca-ses with primary LMS of the kidney that achieved long-term survival up to 70 months after being submitted to radical nephrectomy and concurrent adjuvant chemotherapy and radiotherapy (15). However, surgery may have provided a comple-te cure in this patient. It is therefore likely that adjuvant chemotherapy and radiotherapy may have been an unnecessary procedure. There are re-ports in the literature demonstrating the survival benefits of neoadjuvant chemotherapy in LMSs. Kamba et al. showed that LMS could become re-sectable with the administration of neoadjuvant chemotherapy with CYVADIC (cyclophosphami-de, vincristine, adriamycin, and dacarbazine) (16). There are reports on cases with LMS that achieved an incomplete response with the combination of anti-metabolite gemcitabine and mTOR blocker rapamycin (17). In addition, phase II studies repor-ted the possibility of treating LMS with tyrosine kinase inhibitors such as sunitinib (18).
In their study, Deyrup et al. demonstrated the relationship between increasing histological grade of the renal LMS and survival. The histo-logical grade was defined as a poor prognostic factor (19). Compared to the subtypes of other re-nal malignancies, primary LMS of the kidney is associated with considerably poor prognosis. The correct diagnosis and proper management of the disease requires detailed morphological analysis and careful interpretation of the immunohisto-chemical markers (20). In the literature, the Ki-67 proliferation index ranged from 6% to 50% in LMS (21). The Ki-67 proliferation index in our se-ries of patients is parallel to that reported in the literature. The studies in the literature found that p16 and p53 tumor suppressor proteins are over-
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-expressed in LMS, and therefore could be used as a prognostic marker (22, 23). Unlike many other soft tissue tumors, the genetic basis of LMSs has been poorly understood. LMSs are known to be genetically complex, often showing ‘chaotic’ ka-ryotypes including aneuploidy or polyploidy, and no recurrent tumor-specific translocations have been detected (24). Some soft tissue sarcomas are also encountered in patients with EBV, AIDS, and post-transplant patients (24).
CONCLUSIONS
Primary LMS of the kidney is a smooth muscle tumor with complex genetic and molecu-lar basis exhibiting aggressive biological beha-vior and poor prognosis. The life expectancy in high-grade primary LMS of the kidney is shorter compared to low-grade tumors. It must be kept in mind that mean survival is shorter in patients with high-grade primary LMS, and these patients will die within two years. The elucidation of the biological behavior, molecular and genetic basis of this tumor, and mutagenic factors triggering the disease will increase the understanding of this cancer. Currently, the genetic basis of this tumor is described as “chaotic”. However, the primary goal should be the elucidation of the molecular and genetic basis of the cancer. The discovery of new agents other than gemcitabine and docetaxel is required in order to prolong mean survival in metastatic disease. The data presented in this stu-dy contribute to the understanding of high-grade primary renal leiomyosarcoma and may help in the development of an optimal therapeutic strate-gy to treat high-grade primary renal leiomyosar-coma .The only effective means of therapy is the complete resection of the tumor with wide surgical margins. Other than the surgical complete resec-tion, tumor grade and diameter are the important prognostic factors in primary LMS of the kidney.
ABREvATIONS
LMS = LeiomyosarcomaLMSs = LeiomyosarcomasCTx = ChemotherapyRTx = radiotherapy
CK = CytokeratinEMA = Epithelial membrane antigenSMA = smooth muscle actinBcl-2 = B-cell lymphoma-2HMB45 = Mouse anti Human melenoma antibo-dy-45EBV = Epstein–Barr virüsFH = fumarate hydrataseRCC = Renal cell carcinomaNCI = National Cancer InstituteFNCLCC = French Federation of Cancer Centers Sarcoma GroupAJCC = American Journal of Climate ChangeCYVADIC = cyclosphosphamide, vincristine, adriamycin and dacarbazine
CONFLICT OF INTEREST
None declared. REFERENCES
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_______________________Correspondence address:
Hakan Öztürk, MDBasmane Hospital of Sifa University
Fevzipasa Boulevard No: 172/2, 35240Basmane-Konak-Izmir/Turkey
Fax: + 90 232 446-0770E- mail: [email protected]